This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Abstract

Most of the human herpesviruses can be found in semen, although the reported prevalence
varies considerably between individual studies. The frequent presence of herpesvirus
in semen raises the question whether sexual transmission of the virus could have an
impact on human reproduction. Only few studies have associated seminal shedding of
herpesviruses with impaired sperm quality, reduced fertility, or reduced chances of
pregnancy, whereas most studies fail to find an association. Taken together, no firm
evidence is so far linking the presence of herpesviruses in semen to impaired human
reproduction.

Keywords:

Introduction

It is well established that many pathogens may cause sexually transmitted diseases
(STD). Examples include bacterial infections with Chlamydia trachomatis, Neisseria gonorrhoeae, and Treponema pallidum, which may impair fertility or cause severe congenital disorders. Also viral infections
with herpes simplex virus type 2 (HSV-2), causing genital herpes, or human immunodeficiency
virus (HIV), which untreated may lead to AIDS, are significant health care issues.
It is generally believed that transmission of pathogens causing STD occurs through
direct contact between mucous membranes, however accumulating reports have indicated
that several bacteria [1,2] and viruses, including HIV [3], human papillomavirus (HPV) [4], hepatitis B virus [5], hepatitis C virus [6], Ebola virus [7], adenovirus [8], and various human herpesviruses (HHV) are present in semen. This suggests that semen
may also be an important transmission route, although its precise role can be difficult
to establish. This review will focus on herpesviruses in semen and their potential
significance for human reproduction.

The family of Herpesviridae consists of nine structurally similar, large, enveloped DNA viruses, which all share
the ability to persist latently in the host cell and give rise to recurrent infections.
The HHV have been divided into three subfamilies (α, β, and γ) based on both virological
and biological properties, including the type of primary target cells and the site
of latency. No studies today have examined the individual prevalence of all nine HHV
in semen. The individual studies are summarized in Table 1 (α- and γ-HHV) and Table 2 (β-HHV).

Herpes simplex virus-1 and -2

HSV-1 and -2 are neurotropic α-HHVs. HSV-1 is primarily associated with oral transmission
and recurrent oral lesions, whereas HSV-2 is the major cause of genital herpes, although
both viruses are capable of infecting any region of the body. Primary or recurrent
infections can occur either symptomatically or asymptomatically. The seroprevalence
of HSV-1 and HSV-2 increases with age in both Europe and the USA, reaching a plateau
around age 40 with a prevalence of approximately 70% for HSV-1 and 40-60% for HSV-2
in “high-risk” populations and 20-35% for HSV-2 in “low-risk” populations [41]. The prevalence of HSV-1 is roughly similar in Europe and the USA, whereas the prevalence
of HSV-2 is considerable higher in the USA [41]. Frequently, studies have not discriminated between HSV-1 and -2; in these cases,
we refer to HSV-1/2. HSV-1/2 is sexually transmissible [42], and mother-to-child transmission occurs in 1:1,400-30,000 births, occasionally causing
a life threatening generalized infection in the new-born child [43].

The prevalence of HSV-1/2 in semen varies substantially between different studies
(Table 1). More than half of the studies have reported frequencies of less than 4% in both
fertile and infertile men, but particularly studies from Greece [17] and Russia [13] find, using nested PCR and in situ hybridization, respectively, that almost half
of the semen samples from fertility-clinic attendants contain HSV-1/2. Moreover, also
using nested PCR a study from Japan [15] found HSV-1/2 in semen from 24% of fertility-clinic attendants, but none in semen
from their fathers. Whether these significant variations in prevalence are due to
methodological differences, or reflect a true variation between study populations
may require additional analyses to solve. Out of four studies, three found the parameters
in routine sperm analyses to be normal in sperm from HSV-1/2 positive men or in sperm
exposed to HSV-1/2 in vitro [11,23,44]. The fourth study found that the presence of HSV-1/2 was associated with low sperm
count and poor motility [17]. Indeed, HSV-2 isolated from the testis of a dead man has been reported infectious
[45], and one case of HSV-2 transmission through donor semen to a recipient, who subsequently
acquired a primary infection, has also been reported [42]. Moreover, Bocharova et al. [13] have reported that HSV-2 can be internalized into the heads of morphological normal
and motile sperm, suggesting a potential effect of HSV on pregnancy and outcome. Other
groups have not yet confirmed this interesting observation.

Taken together, the data so far do not suggest that HSV-1/2 is involved in impaired
fertility. Besides from a study of transmission by insemination, the mucosa-associated
HSV-1/2 transmission makes it difficult to estimate the risk of HSV-1/2 transmission
in semen per se. If an association with sperm heads is a general feature of HSV-2,
this might have implications for infection of the endometrium, and warrants additional
investigations to clarify.

Varicella-zoster virus

Varicella-zoster virus (VZV) is an α-herpesvirus infecting most unvaccinated people
during early childhood. Primary infection manifests itself as a usually benign childhood
disease, varicella (chicken pox), whereas reactivation results in zoster (shingles).

Only few studies have investigated the potential presence of VZV in semen. Except
for one study from Greece [23], there is agreement that VZV is neither present in semen from fertility-clinic attendants
(Germany) [11], nor from men of couples undergoing IVF treatment (Spain) [22], or from healthy sperm donors (Denmark) [18]. Taken together, the evidence indicates that VZV is not present in semen, perhaps
reflecting the infrequency of VZV reactivation occurring from the ganglia rather than
immune cells.

Epstein-Barr virus

Epstein-Barr virus (EBV) is a γ-herpesvirus that is primarily B-lymphotropic, although
it may also infect and replicate in epithelia cells in vivo. The age of acquisition
of EBV (measured by antibodies) varies in different geographic areas. When acquired
in early childhood, the infection is usually asymptomatic, whereas primary infection
during puberty may cause infectious mononucleosis. The transmission during puberty
involves saliva with high-titered EBV, but might also be transmitted through genital
secretions, probably through cell-associated EBV [27,46]. EBV can be present in cervical cells [27] and can be transmitted from mother-to-child in approximately 3% of EBV PCR positive
mothers [47]. It has not been reported whether the presence of EBV might impair endometrium receptivity.

An association with leukocytospermia and an increased mean sperm count have been reported
in EBV-positive semen samples [11,23], whereas others do not find an impact on sperm count or motility [17]. Anyhow, it is not known whether the prevalence of EBV in semen of infertile and
fertile men differs. Separate studies on sperm donors and fertility-clinic attendants
demonstrate variations in prevalence between studies from 0.4 to 45% (Table 1). A recent study found significantly increased prevalence of EBV in semen and blood
of HIV-infected individuals. Even in cases with no detectable EBV in the blood, EBV
was present in semen suggesting compartmentalized reactivation [20].

In conclusion, it has not been convincingly demonstrated that EBV in semen impairs
sperm function. Estimates indicate that sexual transmission is a minor route of infection,
but the demonstration of EBV in cervical cells may warrant further investigation of
a potential role of EBV during reproduction.

Human herpesvirus 8

HHV-8, also known as Kaposi’s Sarcoma-Associated Herpesvirus or KSAV, is a γ-herpesvirus
that primarily, but not exclusively, infects B cells. Infection with HHV-8 is predominantly
seen in certain geographic regions in Africa and South America, but this is usually
among older adults. The infection is also observed in immunosuppressed individuals,
but is rare in healthy individuals from North America, North Europe and Asia. Not
surprisingly, most studies have therefore failed to detect HHV-8 in sperm from healthy
donors or fertility-clinic attendants (Kaspersen et al., unpublished observation and
[11,19]). In contrast, Bagasra et al. reported HHV-8 in 2 of 45 semen samples from HIV-negative
men, but further demographic information on these men was not provided. However, HHV-8
was found in semen samples from 64 of 73 (88%) HIV-positive homosexual men. HHV-8
in semen was present in both sperm and mononuclear cells [10]. The prevalence of HHV-8 in previous studies have ranged from 0 to more than 90%,
which may reflect methodological differences (including sensitivity and PCR contaminations),
differences in HIV status, or geographic and population-based differences (see ref
[48], and references herein).

Human cytomegalovirus

HHV-5 or human cytomegalovirus (HCMV) is a β-herpesvirus to which seroconversion occurs
throughout life. Infection by HCMV is often asymptomatic, but clinically important
infections occur in immunocompromised individuals or in pregnant women that subsequently
may give birth to a child with congenital infection. Severe congenital HCMV infection
is associated with growth retardation, mental retardation, deafness, microcephaly,
hepatosplenomegaly, chorioretinitis, calcification, and neurologic impairment (for
review, see Revello and Gerna [49]).

It has been almost four decades since HCMV was first reported in semen from American
men of various populations [50]. Since then, numerous reports on identification of HCMV in semen from differently
defined population groups have accumulated. The majority of these studies report a
prevalence of approximately 6% in men from Germany, North America, France, Africa,
Greece, Denmark, Australia, and Russia (Table 1). In contrast, several studies on semen of fertility-clinic attendants from China,
Taiwan, Spain, and Greece, have reported high prevalences of HCMV between 21.6% to
56.9% [14,22,23,38,40]. This could possibly be explained by geographic variation, however another study
from Greece, also of semen from fertility-clinic attendants, found HCMV in only 7.1%
[17]. Both Greek studies used PCR for HCMV DNA detection; the study that detected the
lower frequency even used nested PCR [17]. Shedding of HCMV in semen is also relatively high in homosexual men [24,39]. Howard et al. found shedding of HCMV in 20 out of 24 HIV-positive, homosexual men
(83.3%), but only in 4 out of 115 healthy donors (3.5%) [16].

Although one case of hematospermia has been associated with HCMV shedding [51], most groups have found the sperm parameters to be unaffected by HCMV [8,11,17,23,31,32,40,44], and two studies that directly compare the prevalence of HCMV in semen from fertile
and infertile men find similar frequencies within the two groups [37,50].

HCMV in semen may be infectious [20,24,39], and HCMV has also been isolated from human endometrial cells [52], suggesting a possible mechanism of direct infection of the endometrial cells by
HCMV carried by sperm. Moreover, productive HCMV infection can be obtained in human
endometrial stroma cells [53]. Since a primary HCMV infection is associated with an increased risk for early abortion
[54,55] and congenital defects in the fetus in general [56], HCMV in semen remains a potential risk of viral transmission, even though this may
be an infrequent route of infection.

Whether HCMV directly impairs sperm fertility has been investigated by Eggert-Kruse
and coworkers [32]. From subfertile couples, semen from 170 males and endocervical material from 156
females were screened for the presence of HCMV by nested PCR. The presence of HCMV
was not concordant between couples, emphasizing that sexual transmission of HCMV is
not a frequent route of infection. Furthermore, no significant correlations between
HCMV and semen quality or between cervical HCMV-infection and mucus quality or female
infertility factor were seen.

In conclusion, sexual transmission of HCMV is rare, but semen may contain infectious
virus with the potential of initiating a primary infection. However, there is no evidence
that HCMV in semen impairs fertility [32]. Longitudinal studies on pregnancy outcome in HCMV-positive versus HCMV-negative
patients are, however, lacking.

Human herpesvirus 6A/B

Closely related to HCMV, the β-herpesviruses HHV-6A and HHV-6B are frequently examined
by methods that do not allow a distinction between the two viruses. Infection usually
occurs in the first years of life giving rise to the childhood disease exanthem subitum,
and most adults in the Western world are seropositive. HHV-6B has tropism for mononuclear
cells, primarily T cells, but is usually found in saliva, which is thought to be the
major route of transmission.

Only few reports are available on the prevalence of HHV-6A/B in human semen. Bezold
et al. found the prevalence to be 4.0% in a German population of infertility patients
[11] and 3.7% in a population of American infertility patients [12]. Chen et al. found HHV-6A/B in 2.0% of infertility patients from China [14], whereas Michou et al. detected HHV-6A/B in 8.2% of 109 men from couples undergoing
IVF treatment in Spain [22]. A slightly higher prevalence of 13.5% was seen by Kaspersen et al. in semen from
Danish sperm donors [18] (Table 2), suggesting that the prevalence of HHV-6A/B is not increased among patients attending
a fertility clinic. A remarkably high prevalence of 66.8% among men attending a fertility
clinic on Crete has been reported by Neofytou et al. using nested PCR [23]. The discrepancies in HHV-6A/B prevalence are most likely not due to geographic or
population-based differences, since HHV-6A/B appears to be present in all the populations.
The most likely explanations are therefore that the nested PCR procedure of Neofytou
et al. might be more sensitive or was contaminated. Nonetheless, it is clear that
HHV-6A/B does not directly affect sperm parameters [11,23]. Interestingly, HHV-6A/B is associated with the acrosome of the sperm [18], but it is not known whether this provide a mechanism for infecting the endometrium.

The binding of HHV-6B to the acrosome [18] suggests that HHV-6B may be transmitted to the uterus by the sperm, but at the same
time this may argue against infection of the oocyte during normal fertilization, since
the acrosome is dissolved prior to the sperm enters the egg. Nevertheless, HHV-6A/B
integrates chromosomally at a frequency of 0.8% [57], and it remains unknown how this integration might happen. Thus, it is expected that
PCR-based detection should identify approximately 1% of semen samples simply due to
chromosomal integration of either HHV-6A or HHV-6B.

In conclusion, there is no evidence so far to indicate that HHV-6A/B affects sperm
function or other aspects of human reproduction, although a potential role of HHV-6A/B
on the endometrium has not been resolved yet.

Human herpesvirus 7

HHV-7 is a β-herpesvirus closely related to HHV-6A and HHV-6B. HHV-7 is usually acquired
prior to age 5, and seroprevalence in adults reaches 96% [58]. Infection by HHV-7 is either asymptomatic or causes exanthem subitum.

Similar to HHV-6A/B, the prevalence of HHV-7 in semen is also based on only few publications.
The prevalence in semen from European sperm donors or men attending a fertility clinic
is similar and within the range of 0.4 to 6.0% (Table 2). HIV-positive men have a slightly higher prevalence, which could be explained by
reactivation of HHV-7 by HIV, although the increase in HHV-7 prevalence is not nearly
at the same level of that seen for HCMV [20]. HHV-7 has been detected in a small percentage of analyzed cervical swaps [59] and in one out of eleven analyzed placental biopsy samples [60], but any association to human reproduction has not been reported. Effects of HHV-7
on sperm parameters have not been evaluated.

In conclusion, there is no evidence to link HHV-7 with human reproduction. It cannot
be excluded that HHV-7 can be transmitted sexually, but the significance of this route,
if any, is unknown at present.

Concluding comments

HSV seroprevalence has been reported higher for a population of female fertility-clinic
attendants compared to a population of pregnant women [61] and high HHV-6A/B antibody titers has been associated with a reduced chance of pregnancy
[62]. Nevertheless, the collective set of data does not indicate an association between
herpesviruses in semen and reduced fertility.

However, if sperm-associated herpesvirus is transmissible to the female cervix or
perhaps even to the endometrium, as has been reported for HSV-2 [42], the consequences may be more difficult to estimate. For instance, the leukemia inhibitory
factor (LIF) cytokine is essential for blastocyst implantation. Mouse LIF-null uteri
are unreceptive, yet LIF-deleted blastocysts are unaffectedly implanted into normally
functioning uteri [63]. Unexplained female infertility is not associated with mutations in the LIF gene
[64]. Hu et al. [65] have shown that the production of LIF is partially regulated by p53 and that p53-null
mice blastocyst implantation rate is significantly reduced. Herpesviruses such as
HSV-1, HCMV, and HHV-6B have the ability to inactivate p53. Thus, implantation of
the blastocyst could hypothetically be negatively influenced by viral infection of
uterus tissue. Although the presence of HHV-6B in cells of the endometrium has not
yet been investigated, it is possible that local infection or reactivation of these
herpesviruses occurs and that viral activity in cells involved in endometrium receptivity
would have a negative effect on human fertility.

Nevertheless, no evidence suggests so far that herpesvirus infection has a negative
influence on reproduction. Indeed pre-pregnancy seropositivity to several viruses
protects against primary infection during pregnancy, decreasing the risk for pregnancy
complications such as preeclampsia [66]. Perhaps maternal infection by certain (herpes) viruses even protects against other
more harmful infections.

The source of herpesviruses in semen has also yet to be determined. It is commonly
known that mumps virus has the potential to infect the testis. Herpesviruses might
share this ability to infect testis tissue. Indeed, EBV and HSV-1 and -2 have been
isolated from human testis, and murine CMV (MCMV) from mouse testis. Additionally,
HSV-2 and HCMV have been identified in prostate tissue, but the effect of herpesvirus
infection at these sites is controversial [67].

Because of the risks of HCMV-mediated congenital defects, the interest for HCMV-screening
on donor semen is increasing. Yet, it is not clear whether HCMV constitutes a threat
to the semen recipient, but since HCMV isolated from semen is infectious [20,24,39], and since purification of HCMV positive semen does not efficiently eliminate the
virus [22], the potential risk of HCMV transmission during assisted reproductive techniques
(ART) cannot be ignored. Serology does not predict the presence of HCMV in semen or
cervix [32], therefore screening of donor semen for HCMV DNA is necessary to prevent the use
of HCMV-contaminated sperm in ART. Unfortunately, this would be costly, because shedding
of herpesviruses fluctuates, necessitating screening of all semen samples rather than
occasional checks [18].